Prostate Cancer Screening With Abbreviated MRI Protocol

Not Applicable

Recruiting

• Conditions: Prostate Cancer
• Interventions: Diagnostic Test: magnetic resonance; Diagnostic Test: serum PSA examination; Procedure: Biopsy

• Registration Number: NCT05603351
• Lead Sponsor: Masaryk Memorial Cancer Institute

Brief Summary

Prostate cancer is one of the most common malignancies in the male population with incidence and mortality rates comparable to breast cancer in women, but in contrast, a population screening program that would fulfill all the recommended criteria is not yet available. According to international recommendations, the preventive PSA sampling used in clinical practice is not suitable because of the concurrent detection of clinically insignificant carcinomas in a major proportion of tests. These clinically non-significant cancers make up a significant and increasing proportion with age. Detection of non-significant cancers burdens the health care system and patients with the care that has no positive impact on their health. Current preventive serum prostate-specific antigen (PSA) testing does not distinguish benign hyperplasia and nonsignificant carcinoma from clinically significant cancer. It is therefore not suitable for full-scale screening.

According to current guidelines, magnetic resonance imaging (MRI) is indicated only in patients with an increased risk of cancer for detection or staging after biopsy and is not used for screening. According to recent studies, MRI has detected an increased proportion of significant cancers in the general population compared to screening based on PSA, while fewer clinically insignificant cancers have been detected. In screening, a shorter examination protocol without contrast medium (biparametric MRI) is used with a lower cost per examination, allowing to increase both the number of patients examined and patient comfort.

The main objective of the project is to assess the contribution of imaging in the screening of clinically significant prostate cancer and to validate the published results in the Czech population, and extend the screening model by the second round of examinations and additional laboratory markers. The secondary aim is to design a subsequent study with a larger number of participants allowing statistical evaluation, similar to the successful breast cancer screening.

Detailed Description

A prospective cross-sectional (with a longitudinal component, 2nd screening round) study evaluating the possibility of using the biparametric MRI protocol technique for screening clinically significant prostate cancer in men from the general population.

Tests performed:

* Serum PSA

* PHI calculation (Prostate Health Index) to be performed only if the PSA values are in the range of 2-10 ng/l

* MRI of the prostate (abbreviated biparametric protocol)

* Digital rectal examination (DRE) as part of a clinical visit at a urologist in patients with a positive PSA test

* Biopsy - if indicated

MRI specifications:

* Protocol with anatomical T2 sequence and diffusion-weighted images (DWI), according to the standards

* Typical complete examination time does not exceed 20 minutes, planned acquisition time less than 15 minutes.

* No contrast agent or spasmolytics is injected.

Blinding:

* Every test evaluator (radiologist/urologist) does not know the results of other tests. · MRI reports entered in the registry obligatorily before the biopsy.

* The patient is not informed which test was positive and resulted in an indication for biopsy.

* The pathologist does not know the results of MRI or laboratory tests.

The sequence of tests:

The MRI is assessed with the PI-RADS 2.1 system, each finding is reported on a scale of 1-5. To minimize the detection of non-significant cancers and to reduce the number of biopsies according to the results of the IP1-Prostagram study, a PI-RADS value of 4-5 was chosen as a positive test representation.

Consensual double reading by 2 experienced uroradiologists (at least 400 MRI of the prostate read by the beginning of the study). Men with a positive MRI test are planned for a targeted MRI/US fusion and systematic prostate biopsy.

Men with a positive blood marker (either PSA, PSAD, or PHI) are planned for a systematic 12 core biopsy. Positive test results are PSA ≥ 3, integrated marker PSAD ≥ 0.15, and PHI ≥ 35.

Study participants are invited to repeat the screening tests after 2 years by letter. If they do not respond to a written offer, also by e-mail and SMS.

Definition of clinically significant cancer: • ISUP Grade Group ≥ 2.

Study Timeline

• Study Start: 2022-05-01
• Study First Submitted: 2022-09-02
• Status Verified: 2022-10
• Study First Submitted QC: 2022-10-30
• Last Update Submitted: 2022-10-30
• Study First Posted: 2022-11-02
• Last Update Posted: 2022-11-02
• Primary Completion: 2025-06-30
• Study Completion: 2025-12-31

Recruitment & Eligibility

• Status: RECRUITING
• Sex: Male
• Target Recruitment: 300

Inclusion Criteria

• Age 50-69 years
• Life expectancy over 10 years
• Ability to undergo all planned procedures (without contraindications to MRI or biopsy)
• No known prostate cancer or prostate biopsy in the past (interventions for BPH are not a restriction)
• No PSA test or prostate MRI in the past 2 years.
• No signs of prostatitis or urinary tract infection in the past 6 months.
• Signed informed consent.

Exclusion Criteria

• Contraindications to MRI
• Hip replacement
• Known BRCA1/BRCA2 mutation

Study & Design

• Study Type: INTERVENTIONAL
• Study Design: SINGLE_GROUP

Arm && Interventions

Group	Intervention	Description
Preventive prostate examination by bpMRI	serum PSA examination	The cohort consists of patients: * with age 50-69 years * without any contraindications to MRI or biopsy * without known status of prostate cancer or prostate biopsy in the past (interventions for BPH are not a restriction) * without known BRCA mutation * without PSA test or prostate MRI in the past 2 years * without any signs of prostatitis or urinary tract infection in the past 6 months.
Preventive prostate examination by bpMRI	magnetic resonance	The cohort consists of patients: * with age 50-69 years * without any contraindications to MRI or biopsy * without known status of prostate cancer or prostate biopsy in the past (interventions for BPH are not a restriction) * without known BRCA mutation * without PSA test or prostate MRI in the past 2 years * without any signs of prostatitis or urinary tract infection in the past 6 months.
Preventive prostate examination by bpMRI	Biopsy	The cohort consists of patients: * with age 50-69 years * without any contraindications to MRI or biopsy * without known status of prostate cancer or prostate biopsy in the past (interventions for BPH are not a restriction) * without known BRCA mutation * without PSA test or prostate MRI in the past 2 years * without any signs of prostatitis or urinary tract infection in the past 6 months.

Primary Outcome Measures

Name	Time	Method
Proportion of positive PI-RADS detections in the cohort of patients indicated for biopsy.	2 years	Ratio of significant and non-significant cancers in individual categories of PI-RADS scores in patients indicated for biopsy.
Assessment of the importance of the imaging test in the screening of significant prostate cancer in asymptomatic men, compared with PSA screening: Proportion of positive MRI findings	2 years	Proportion of positive MRI findings (PI-RADS 4+) in the general population of men aged 50-69 years.
Distribution of PI-RADS scores in the observed cohort.	2 years	Distribution of PI-RADS scores (proportion of individual scores 1-5) in the screened population.

Secondary Outcome Measures

Name	Time	Method
Feasibility evaluation of a larger-scale study of screening for significant prostate cancer using an imaging modality:	2 years	Concordance rate (%) between radiologists performing MRI scoring.
Patient adherence to preventive examination.	2 years	Number of participants who signed the informed consent and were enrolled in the study.
Evaluation of patient adherence to preventive examination.	2 years	Number of participants who visited a screening facility.
Evaluation of complications after an interventional procedure (biopsy).	2 years	Number of complications after biopsy.
Patient adherence to preventive examination - self-recruitment.	2 years	Number of participants who contacted the team themselves with a request for testing.
Evaluation of patient adherence to preventive examination - active recruitment.	2 years	Number of participants who agreed to be included in the study through used recruitment strategies.
Evaluation of patient adherence to preventive examination - completation of planned exams.	2 years	Number of participants who completed the designated examination.
Evaluation of the financial burden of the study for the future preventive program of prostate cancer screening.	2 years	Costs of individual inclusion and screening tests.
Detection and assessment of potential barriers to patient participation in the study. Assessment of patient adherence to remain in the study throughout the study period.	2 years	Numbers and reasons of participants who did not complete scheduled tests, follow-up examinations, or withdrew informed consent.

Trial Locations

Locations (1)

Masaryk Memorial Cancer Institute; 🇨🇿 Brno, Czech Republic, Czechia